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Abstract

Background: Oral squamous cell carcinoma (OSCC) is among the frequently reported malignancies in Pakistan having unfavorable prognosis. Extracellular Matrix Metalloproteinase Inducer (EMMPRIN) is a transmembrane glycoprotein that is implicated in tumorigenesis and is recognized as a potential therapeutic target in multiple carcinomas.

Objective: To determine the immuohistochemical expression of EMMPRIN (CD147) in biopsies from OSCC patients in the Pakistani population.

Methods: This descriptive study was conducted in Lahore, Pakistan, comprising 100 OSCC cases presenting, from January 2010 to September 2015. Detailed clinical parameters were recorded. Histological diagnosis & grade was assessed followed by scoring of CD147 immunoexpression into low (score 0-5) and high (score 6-7). The data were analysed using SPSS 21.0. Pearson Chi square and Fisher Exact test were applied. A P value ≤0.05 was considered as statistically significant.

Results: Histologically, conventional OSCC was the most prevalent subtype (92%) followed by oral papillary (6%) and verrucous (2%) carcinomas. Well differentiated carcinomas made most of the tumour burden (64%). 60% carcinomas expressed high score while 40% showed low expression scores. EMMPRIN expression was significantly associated with the degree of differentiation of the tumour (P=0.001).

Conclusions: The findings of the current study highlight the significance of EMMPRIN (CD147) expression in relation to cancer progression thus marking its potential for being an attractive target for immunotherapeutic approaches.

Introduction

Oral squamous cell carcinoma (OSCC) is globally one of the most frequently reported malignant neoplasms, accounting for more than 90% of oral cancers. In Pakistan, it is the second most common malignancy [1] and comprises 15% of estimated new cancer cases in this region compared to 3% detected worldwide [2].

OSCC demonstrates histologically a heterogeneous cell population with differences in the degree of differentiation, invasive and metastatic potential. The mortality and morbidity of OSCC has not changed considerably over the last few decades. Detection of biomarkers implicated in various cancers and the advent of targeted molecular therapies have led to a radical change in the treatment of different tumours.

Extracellular matrix metalloproteinase inducer (EMMPRIN), also known as CD147, was originally identified as a tumour cell membrane protein that induces matrix metalloproteinase (MMP) production from adjacent fibroblasts [3]. It is present both on the tumour and normal cells and it is believed to play major roles in the regulation of different cellular activities. EMMPRIN expression is enhanced in several malignancies as compared to benign and the normal tissues [4]. Overexpression or mutation of EMMPRIN is found in 95% of the patients with oral SCC [5]. It plays a vital role in the tumorigenesis by promoting invasion, angiogenesis, growth and survival of malignant cells because of its association with different proteins involved in various signalling pathways [5].

Recently, EMMPRIN (CD147) has been reported to be a useful diagnostic and prognostic marker as it is involved in various aspects of cancer progression [6]. The current study aimed at determining, for the first time in Pakistan, the immuohistochemical expression of EMMPRIN in patients with oral squamous cell carcinoma and to investigate the association of this protein with various clinicopathological parameters of the tumour in our population.

Materials and methods

This descriptive study was conducted at the Department of Oral Pathology, Lahore, Pakistan. Approval from the institutional ethical review committee was obtained prior to the commencement of the study. A total of 100 biopsies of patients who reported with various histological subtypes and grades of OSCC from both genders and all age groups were included. While patients already on chemo-radio therapy and/or with recurrence were excluded. All selected patients gave written informed consent. Relevant demographic and clinical information were collected from departmental record. The tissues were processed for making paraffin blocks and sections were cut and stained with haematoxylin and eosin for confirmation of the histological diagnosis and grading/ subtyping of tumours. The histological grading of conventional OSCC and papillary OSCC was undertaken according to the criterion laid by Bryne et al. [7] and Velazquez et al. [8] respectively, while oral verrucous carcinoma was taken as well differentiated by default [9].

ImmunohistochemistryAbout 4 μm thick tissue sections were cut with the help of rotary microtome and mounted on Poly-L-lysine coated slides. Sections were deparaffinised in xylene and rehydrated in graded ethyl alcohol, followed by immersion in citrate buffer solution of pH 9.0 and were put in the hot water bath before staining procedures. Immunohistochemistry was performed using the standard ‘Streptavidin biotin Peroxidase’ method. Sections were then incubated with mouse IgG1 kappa primary monoclonal CD147 antibody [HIM6] (Bio Legend; USA) with a dilution of 1:25 and DAB chromogen was applied to the sections followed by counterstaining with haematoxylin. Positive (oral mucosa and skin) and negative (omission of primary antibody) controls were run with each batch of 20 histological sections of OSCCs. EMMPRIN (CD147) expression was scored on basis of proportion and intensity of immunolabeling in tumour cell membrane and cytoplasm.

Statistical analysisThe data were entered and analysed using SPSS 21.0. Mean±S.D were given for quantitative variables and frequencies and percentages were computed for qualitative variables. Pearson Chi square and Fisher Exact test were applied to observe associations between the variables. A P value ≤0.05 was considered as statistically significant.

Results

Of the 100 OSCC cases, the overall mean age of the patients was 51.28±15.65 years with the age range of 25-80 years. The male to female ratio was 1.3:1 with most cases reported in 5th to 6th decade of life (Table 1).

Variable clinical presentations were recorded in all study cases (Table 2). As regards the site of involvement of oral cavity, occurrence of OSCC was higher on the tongue (40%) followed by buccal mucosa (34%) and other sites (Table 2). In females, predominant involvement of tongue was seen (43%) whereas in males, buccal mucosa was the most commonly involved site (41%).

Table 2 : Clinical Presentation and Gender Distribution with respect to Site in OSCC.

In the current study, the most prevalent histological subtype was conventional oral squamous cell carcinoma (92%). This was followed by oral papillary (6%) and verrucous (2%) carcinomas (Table 3). Regarding the histological grades, well differentiated OSCC was the most common presentation in the present study patients (Table 3).

EMMPRIN high and low expression scores in different histological grades of OSCC (Table 4) demonstrate that cases of moderate and poorly differentiated OSCC exhibited high expression score more often than well differentiated tumours (P=0.001). However, no significant association between EMMPRIN expression and the other listed clinicopathological variables was seen.

Table 4 : Association of EMMPRIN (CD147) expression with different clinicopathological features of OSCC Cases.

Discussion

Oral carcinogenesis is a multistep cascade that involves complex molecular pathways in disease progression. Targeting the molecular pathways involved in tumorigenesis remains the greatest opportunity to halt cancer progression. In the present study, among the 100 OSCC cases evaluated for different clinicopathological variables, the mean age of occurrence (51.28±15.65 years) is consistent with the study conducted by Rahman et al. [11] with most cases seen in the fifth decade of life.

The gender related findings of the current study (Male: Female ratio, 1.3:1) are also consistent with the local [12] and international studies [13] showing male predominance. In the current study, the commonest presenting complaint was non healing ulcer (48%) with the tongue being the most frequently affected site (40%). These finding are in accordance with other studies [14].

As regards the histologic subtypes, conventional OSCC was the most prevalent subtype encountered in the current study (92%); and this finding is almost universal in all local and international studies. The clinical variables, age, site of tumour, gender and clinical presentation in conventional OSCC are found to be similar to the parameters of OSCC as discussed earlier.

The papillary OSCC was diagnosed in 6% of the present cases, while Thompson [15] revealed that it constitutes approximately 1 % of all OSCCs. In contrast to the findings of the current study, Bao et al. [16] reported 63.3 years mean age and found the most frequent site to be the gingiva. Most studies have demonstrated that papillary OSCC shows male predilection and presents clinically as an exophytic mass [17], a finding corroborated by the present results.

Verrucous carcinoma (VC) accounted for 2% of the total studied cases of the present study. Neville et al. [18] reported that VC accounts for 1-10% of all oral squamous cell carcinomas, depending on the local acceptance of smokeless tobacco use. In the current study, VC clinically presented at an age of 65 years as an exophytic mass on the buccal mucosa, which is in accordance with the reviewed literature [19].

As for the histological grade, among the 100 OSCC cases investigated, well differentiated carcinomas made most of the tumour burden (64%). Among 92 cases of conventional OSCC, most of the cases were well differentiated (67.4%) followed by moderate and poorly differentiated cases. Comparable results were seen in local [12] and international studies [20].

In the present study, verrucous carcinoma was taken as well differentiated by default [9].

Regarding papillary OSCC, all the cases in the present study were graded as moderately differentiated. However, in the study conducted on gingival papillary SCC, Fitzpatrick et al. [21] demonstrated most of the cases as either well or moderately-well differentiated (88%) while 12 % of the cases were graded as moderate or moderately-poor. Such variations in OSCC could be attributed to ethnic and racial disparities and can be closely related to prognosis.

In the current study, EMMPRIN immunohistochemical expression was evaluated in OSCC cases presenting in our part of the world. All studied cases of OSCC (100%) were positive for CD 147 antibody with EMMPRIN (CD147) immunoexpression seen predominantly in tumour cell membrane (Figure 2B) and also in cytoplasm (Figure 2A) of some cases. This is in accordance with the immunohistochemical studies done by Piao et al. [10] in salivary duct carcinoma. Cytoplasmic and membranous staining pattern acquired by tumour cells may be attributed to cytoplasmic and membranous domain of EMMPRIN (CD147), as described by Iacono et al. [22].

According to the immunostaining results of the present study, more than half of the OSCC cases (60%) were categorized as having high EMMRIN expression score and (40%) cases showed low EMMPRIN expression scores. No case was detected showing negative staining. Similar to these findings, Monteiro et al. [5] showed positive EMMPRIN (CD147) immunoreactivity in all examined OSCC cases with high expression in 75.7% of the cases.

However, the positive control specimens (normal skin and buccal mucosa), investigated in the present study, depicted no strong positive staining with enhanced EMMPRIN staining in the basal cell layer suggesting the proliferative potential of EMMPRIN (CD147) (Figure 1). This is in compliance with the findings of Huang et al. [23], who demonstrated a significantly higher expression in cancer cells compared with adjacent non-cancerous epithelium in tongue squamous cell carcinomas. Even though EMMPRIN (CD147) showed weak positivity in normal epithelial cells, it might be representative of a physiological role in tissue remodelling under specific conditions [24].

In the present study, no significant association was instituted between EMMPRIN (CD147) immuno-histochemical expression and different clinical parameters of OSCC (age, gender, site, clinical presentation) which is consistent with other studies [5,25]. Moreover, relation between EMMPRIN expression and histologic subtypes of OSCC was also found to be statistically insignificant (P>0.05). This can be due to varying morphologic features and biological behaviour of different histological subtypes. However, we found significant association (P=0.001) between the low and high EMMPRIN scores and histological grades of OSCC, where moderate (77%) and poorly differentiated (100%) OSCCs exhibited high expression score as compared to well differentiated tumours (47%). Studies focused on EMMPRIN high and low score [5,25] are concordant to the findings of the present study demonstrating significant association of EMMPRIN expression with histological grades of OSCC (P=0.002 & 0.005 respectively).

In contrast to these findings, the study conducted by Huang et al. [23] on tongue squamous cell carcinoma reported no significant association between EMMPRIN (CD147) expression and histologic grades (P=0.962). These discrepancies suggest different grouping and statistical methods and might be largely attributable to different governing mechanisms of EMMPRIN (CD147) expression in cells of different origin.

Since EMMPRIN (CD147) is a multifunctional biological molecule and an important factor in epithelial connective tissue interactions, it is likely to play an important role in OSCC progression. Previously, Baba et al. [26] reported that blocking CD147 using monoclonal antibody induces cell death in cancer cells of colon cancer. Thus EMMPRIN (CD147) might be considered as an objective and effective marker to predict the invasion and prognosis of OSCC.

To our knowledge, no such documented immunohistochemical study elaborating the role of Extracellular Matrix Metalloproteinase Inducer (EMMPRIN) in OSCC has been conducted in Pakistan or any other South Asian country so there is a lack of data for comparison in this regard. Further studies on larger sample size are required to explicate the molecular and genetic mechanisms to assess the tumour related effects of EMMPRIN (CD147). Better understanding of the molecular mechanisms causing dysregulated growth and OSCC progression may provide a basis for discovering new treatment modalities and can be useful in the development of new molecular therapies and targeting tools. This area of future research undoubtedly will further improve our understanding of OSCC carcinogenesis and the role played by EMMPRIN (CD147).

Conclusion

EMMPRIN (CD147) protein is widely but variably expressed in all OSCC cases in our population, with a significant association with the degree of differentiation of the tumour.

The findings of the current study highlight the significance of EMMPRIN (CD147) expression in relation to cancer progression thus marking its potential for being an attractive target for immunotherapeutic approaches.

Acknowledgement

The authors acknowledge the encouragement extended by the Vice Chancellor of University of Health Sciences, Lahore Pakistan. Also, to Mr. Sameer Anjum and Mr. Ghulam Rasool, the laboratory staff of Morbid Anatomy & Histopathology Department, University of Health Sciences, Lahore, Pakistan for their technical and logistic support.